LBPO.CH01 · 化学 · Late-Breaking
Preclinical evaluation of a novel orally bioavailable MDM2 PROTAC, NW-8-461, in acute leukemia and myelofibrosis
作者与单位
摘要 Abstract
Murine double minute 2 (MDM2) is a key negative regulator of the tumor suppressor p53 and is frequently overexpressed or amplified in p53-wild-type cancers, resulting in functional suppression of p53 signaling. Although small-molecule inhibitors that disrupt the MDM2-p53 interaction have demonstrated clinical activity, their efficacy is limited by on-target toxicity, incomplete pathway inhibition, and resistance driven by sustained MDM2 protein expression. Proteolysis-targeting chimeras (PROTACs) offer a novel therapeutic strategy by inducing selective and catalytic degradation of target proteins. Here, we describe NW-8-461, a potent MDM2-targeting PROTAC that induces efficient MDM2 degradation with a DC₅₀ <1 nM and robust activation of p53 signaling in RS4;11 leukemia cells. NW-8-461 exhibits markedly enhanced antiproliferative activity, demonstrating approximately 10-fold and 100-fold greater potency in cell viability assays compared with RG7388 and AMG232, respectively. Consistent with a p53-dependent mechanism, NW-8-461 selectively inhibits cell viability in myelofibrosis cell lines harboring wild-type p53 but not mutant p53. Notably, at 1 µM, NW-8-461 shows minimal or no degradation of key off-target proteins, including IKZF1, IKZF3, SALL4, GSPT1, and CK1alpha, indicating high target selectivity. In mice, NW-8-461 demonstrates favorable pharmacokinetics and oral bioavailability, achieving a plasma C_max of 9,660 ng/mL following a single oral dose of 50 mg/kg. In an orthotopic RS4;11-Luc leukemia model, treatment with NW-8-461 at 25 mg/kg for 16 days resulted in complete eradication of leukemia cells in 7/7 mice and significantly superior efficacy compared with the MDM2 inhibitor RG7388. These results establish NW-8-461 as a differentiated and highly selective MDM2 degrader with strong therapeutic potential for p53-wild-type malignancies.
利益披露 Disclosure
Q. Zhang,
Guangzhou Lupeng Pharmaceutical Company Employment.
Y. Xu,
Guangzhou Lupeng Pharmaceutical Company Employment.
Q. Wu,
Guangzhou Lupeng Pharmaceutical Company Employment.
C. Z. Tu, None..
S. Wang, None.
K. Yin,
Guangzhou Lupeng Pharmaceutical Company Employment.
X. Xu,
Guangzhou Lupeng Pharmaceutical Company Employment.
Z. Zhang, None.
B. Dai,
Guangzhou Lupeng Pharmaceutical Company Employment.
F. Tan,
Guangzhou Lupeng Pharmaceutical Company Employment.
Y. Chen,
Guangzhou Lupeng Pharmaceutical Company Employment.